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从与前列腺癌相关的粪便微生物组中鉴定出的代谢生物合成途径。

Metabolic Biosynthesis Pathways Identified from Fecal Microbiome Associated with Prostate Cancer.

机构信息

Department of Urology, University of Texas Health Science Center, San Antonio, TX, USA; South Texas Veterans Healthcare System, San Antonio, TX, USA.

Resphera Biosciences, Baltimore, MD, USA.

出版信息

Eur Urol. 2018 Nov;74(5):575-582. doi: 10.1016/j.eururo.2018.06.033. Epub 2018 Jul 12.

Abstract

BACKGROUND

The fecal microbiome is associated with prostate cancer risk factors (obesity, inflammation) and can metabolize and produce various products that may influence cancer but have yet to be defined in prostate cancer.

OBJECTIVE

To investigate gut bacterial diversity, identify specific metabolic pathways associated with disease, and develop a microbiome risk profile for prostate cancer.

DESIGN, SETTING, AND PARTICIPANTS: After prospective collection of 133 rectal swab samples 2 wk before the transrectal prostate biopsy, we perform 16S rRNA amplicon sequencing on 105 samples (64 with cancer, 41 without cancer). Phylogenetic Investigation of Communities by Reconstruction of Unobserved States (PICRUSt) was applied to infer functional categories associated with taxonomic composition. The p values were adjusted using the false discovery rate. The α- and β-diversity analyses were performed using QIIME. The Mann-Whitney U test was employed to evaluate the statistical significance of β-diversity distances within and between groups of interest, and least absolute shrinkage and selection operator (LASSO) regression analysis was used to determine pathway significance.

OUTCOME MEASUREMENTS AND STATISTICAL ANALYSIS

The detection of prostate cancer on transrectal prostate needle biopsy and 16s microbiome profile.

RESULTS AND LIMITATIONS

We identified significant associations between total community composition and cancer/non-cancer status (Bray-Curtis distance metric, p<0.01). We identified significant differences in enrichments of Bacteroides and Streptococcus species in cancer (all p<0.04). Folate (LDA 3.8) and arginine (LDA 4.1) were the most significantly altered pathways. We formed a novel microbiome-derived risk factor for prostate cancer based on 10 aberrant metabolic pathways (area under curve=0.64, p=0.02).

CONCLUSIONS

Microbiome analyses on men undergoing prostate biopsy noted mostly similar bacterial species diversity among men diagnosed with and without prostate cancer. The microbiome may have subtle influences on prostate cancer but are likely patient-specific and would require paired analysis and precise manipulation, such as improvement of natural bacterial folate production.

PATIENT SUMMARY

Microbiome evaluation may provide patients with personalized data regarding the presence or absence of particular bacteria that have metabolic functions and implications regarding prostate cancer risk. The study provides a basis to investigate the manipulation of aberrant microbiomes to reduce prostate cancer risk.

摘要

背景

粪便微生物群与前列腺癌的风险因素(肥胖、炎症)有关,并且可以代谢和产生各种可能影响癌症的产物,但尚未在前列腺癌中得到定义。

目的

研究肠道细菌多样性,确定与疾病相关的特定代谢途径,并为前列腺癌开发微生物组风险概况。

设计、设置和参与者:在经直肠前列腺活检前 2 周前瞻性收集 133 个直肠拭子样本后,我们对 105 个样本(64 个有癌症,41 个没有癌症)进行 16S rRNA 扩增子测序。应用重建未观察状态的群落系统发育分析(PICRUSt)推断与分类组成相关的功能类别。使用错误发现率调整 p 值。使用 QIIME 进行 α 和 β 多样性分析。使用 Mann-Whitney U 检验评估组内和组间β多样性距离的统计学意义,使用最小绝对收缩和选择算子(LASSO)回归分析确定途径的显著性。

测量和统计分析结果

经直肠前列腺针活检和 16s 微生物组谱检测前列腺癌。

结果和局限性

我们发现总群落组成与癌症/非癌症状态之间存在显著关联(Bray-Curtis 距离度量,p<0.01)。我们发现癌症中 Bacteroides 和 Streptococcus 物种的丰度存在显著差异(所有 p<0.04)。叶酸(LDA 3.8)和精氨酸(LDA 4.1)是最显著改变的途径。我们根据 10 个异常代谢途径形成了一种新的前列腺癌微生物组衍生风险因素(曲线下面积=0.64,p=0.02)。

结论

对接受前列腺活检的男性进行的微生物组分析发现,诊断为前列腺癌和未诊断为前列腺癌的男性之间的细菌物种多样性大致相似。微生物组可能对前列腺癌有微妙的影响,但可能是患者特异性的,需要进行配对分析和精确操作,例如改善天然细菌叶酸的产生。

患者总结

微生物组评估可为患者提供有关特定细菌是否存在的个性化数据,这些细菌具有代谢功能,与前列腺癌风险有关。该研究为研究操纵异常微生物组以降低前列腺癌风险提供了基础。

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